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3,5-DIMETHOXY-4-(2-PROPYNYLOXY)PHENETHYLAMINE
SYNTHESIS: To a
solution of 5.8 g
homosyringonitrile (see under E for
its preparation) in 50 mL
acetone containing 100 mg
decyltriethylammonium iodide, there was added 12 g of an 80%
solution
of
propargyl bromide in
toluene and 6.9 g of finely powdered
anhydrous
K2CO3. This mixture was held at reflux on the steam bath for 12 h,
after which the
solvent was removed under vacuum. The residues were
added to 0.5 L H2O, acidified, and extracted with 3x75 mL
CH2Cl2. The
extracts were pooled, washed with 5%
NaOH, and then with dilute HCl
which discharged the deep color. Removal of the organic
solvent under
vacuum yielded 6.6 g of crude product. This was
distilled at 138-148
°C at 0.25 mm/
Hg, yielding 4.3 g
3,5-dimethoxy-4-(2-propynyloxy)phenylacetonitrile which spontaneously
crystallized. A small sample from MeOH had a mp of 94-95 °C. Anal.
(
C13H13NO3) C,H.
A suspension of 2.8 g LAH in 70 mL
anhydrous THF was cooled to 0 °C
with good stirring under He, and treated with 2.0 g 100% H2SO4. To
this, a
solution of 4.2 g
3,5-dimethoxy-4-(2-propynyloxy)phenylacetonitrile in 30 mL
anhydrous
THF was added very slowly. After the addition had been completed, the
reaction mixture was held at reflux on the steam bath for 0.5 h,
cooled to room tem
perature, treated with IPA to decompose the excess
hydride, and finally with 15%
NaOH to convert the solids to a white
filterable mass. The solids were separated by filtration, the filter
cake was washed with THF, and the filtrate and washes were pooled.
After removal of the
solvent, the residue was added to 100 mL dilute
H2SO4, and washed with 3x75 mL
CH2Cl2. The aqueous
phase was made
basic with dilute
NaOH, and the product extracted with 2x75 mL
CH2Cl2.
After removal of the
solvent under vacuum, the residue was
distilled
at 125-155 °C at 0.3 mm/
Hg to provide 2.4 g of a light amber viscous
liquid. This was
dissolved in 10 mL IPA, acidified with concentrated
HCl until a droplet produced a red color on dampened, external
universal
pH paper, and then diluted with 40 mL
anhydrous Et2O with
good stirring. After a short delay,
3,5-dimethoxy-4-(2-propynyloxy)phenethylamine hydrochloride (
PROPYNYL)
spontaneously
crystallized. The product was removed by filtration,
washed first with an IPA/
Et2O mixture, and finally with Et2O. The
yield was 3.0 g of white needles.
DOSAGE: 80 mg or more.
DURATION: 8 - 12 h.
QUALITATIVE COMMENTS: (with 55 mg) I have cold feet--literally--I
don't mean that in the spiritual or adventurous sense. But also I am
somewhat
physically fuzzy. I feel that if I were in public my
behavior would be such that someone would notice me. Everything was
OK without any question at the ninth hour. I could walk abroad
again.
(with 80 mg) There is a body load. The flow of people around me all
day has demanded my attention, and when I had purposefully retreated
to be by myself, there was no particular reward as to visuals or
anything with eyes closed, either. Sleep was easy at midnight (the
twelth hour of the experiment) but the morning was sluggish, and on
recalling the day, I am not sure of the events that had taken place.
Higher might be all right, but watch the status of the body. There
certainly wasn't that much mental stuff.
EXTENSIONS AND COMMENTARY: No experiments have been performed that
describe the action of this drug at full level. This compound does
not seem to have the magic that would encourage exploration at higher
levels.
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